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首页> 外文期刊>American Journal of Cancer Research >Microarray expression profiling identifies genes, including cytokines, and biofunctions, as diapedesis, associated with a brain metastasis from a papillary thyroid carcinoma
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Microarray expression profiling identifies genes, including cytokines, and biofunctions, as diapedesis, associated with a brain metastasis from a papillary thyroid carcinoma

机译:微阵列表达谱鉴定出与乳头状甲状腺癌的脑转移有关的基因,包括细胞因子和生物功能,如尿布分离

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摘要

Brain metastatic papillary thyroid carcinomas (PTCs) are afflicted with unfavorable prognosis; however, the underlying molecular genetics of these rare metastases are virtually unknown. In this study, we compared whole transcript microarray expression profiles of a BRAF mutant, brain metastasis from a PTC, including its technical replicate (TR), with eight non-brain metastatic PTCs and eight primary brain tumors. The top 95 probe sets (false discovery rate (FDR) p-value < 0.05 and fold change (FC) > 2) that were differentially expressed between the brain metastatic PTC, including the TR, and both, non-brain metastatic PTCs and primary brain tumors were in the vast majority upregulated and comprise, e.g. ROS1, MYBPH, SLC18A3, HP, SAA2-SAA4, CP, CCL20, GFAP, RNU1-120P, DMBT1, XDH, CXCL1, PI3, and NAPSA. Cytokines were represented by 10 members in the top 95 probe sets. Pathway and network analysis (p-value < 0.05 and FC > 2) identified granulocytes adhesion and diapedesis as top canonical pathway. Most significant upstream regulators were lipopolysaccharide, TNF, NKkB (complex), IL1A, and CSF2. Top networks categorized under diseases & functions were entitled migration of cells, cell movement, cell survival, apoptosis, and proliferation of cells. Probe sets that were significantly shared between the brain metastatic PTC, the TR, and primary brain tumors include CASP1, CASP4, C1R, CC2D2B, RNY1P16, WDR72, LRRC2, ZHX2, CITED1, and the noncoding transcript {"type":"entrez-nucleotide","attrs":{"text":"AK128523","term_id":"34535931","term_text":"AK128523"}}AK128523. Taken together, this study identified a set of candidate genes and biofunctions implicated in, so far nearly uncharacterized, molecular processes of a brain metastasis from a PTC.
机译:脑转移性甲状腺乳头状癌(PTCs)的预后不良。然而,这些罕见转移的潜在分子遗传学实际上是未知的。在这项研究中,我们比较了BRAF突变体的完整转录本微阵列表达谱,PTC的脑转移(包括其技术复制(TR))与8种非脑转移性PTC和8种原发性脑肿瘤。前95个探针集(错误发现率(FDR)p值<0.05和倍数变化(FC)> 2)在包括TR在内的脑转移PTC与非脑转移PTC和原发性PTC之间差异表达脑肿瘤在绝大多数情况下被上调并且包括例如ROS1,MYBPH,SLC18A3,HP,SAA2-SAA4,CP,CCL20,GFAP,RNU1-120P,DMBT1,XDH,CXCL1,PI3和NAPSA。在前95个探针组中,有10个成员代表细胞因子。途径和网络分析(p值<0.05和FC> 2)确定粒细胞粘附和尿布分离是最典型的途径。最重要的上游调节因子是脂多糖,TNF,NKkB(复合物),IL1A和CSF2。归类于疾病和功能的顶级网络称为细胞迁移,细胞运动,细胞存活,细胞凋亡和细胞增殖。在脑转移性PTC,TR和原发性脑肿瘤之间显着共享的探针集包括CASP1,CASP4,C1R,CC2D2B,RNY1P16,WDR72,LRRC2,ZHX2,CITED1和非编码转录本{“ type”:“ entrez-核苷酸”,“ attrs”:{“ text”:“ AK128523”,“ term_id”:“ 34535931”,“ term_text”:“ AK128523”}} AK128523。综上所述,这项研究确定了一组候选基因和生物功能,这些基因和生物功能与PTC引起的脑转移的分子过程有关,迄今为止几乎未表征。

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